4.8 Article

Real-time shape approximation and fingerprinting of single proteins using a nanopore

Journal

NATURE NANOTECHNOLOGY
Volume 12, Issue 4, Pages 360-367

Publisher

NATURE PUBLISHING GROUP
DOI: 10.1038/NNANO.2016.267

Keywords

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Funding

  1. Miller Faculty Scholar Award
  2. Air Force Office of Scientific Research [FA9550-12-1-0435]
  3. Oxford Nanopore Technologies [350509-N016133]
  4. National Institutes of Health [1R01GM081705]
  5. National Human Genome Research Institute [HG003290, HG004776]
  6. University of Michigan
  7. National Science Foundation
  8. Microfluidics in Biomedical Sciences Training Program from NIH
  9. BIBIB

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Established methods for characterizing proteins typically require physical or chemical modification steps or cannot be used to examine individual molecules in solution. Ionic current measurements through electrolyte-filled nanopores can characterize single native proteins in an aqueous environment, but currently offer only limited capabilities. Here we show that the zeptolitre sensing volume of bilayer-coated solid-state nanopores can be used to determine the approximate shape, volume, charge, rotational diffusion coefficient and dipole moment of individual proteins. To do this, we developed a theory for the quantitative understanding of modulations in ionic current that arise from the rotational dynamics of single proteins as they move through the electric field inside the nanopore. The approach allows us to measure the five parameters simultaneously, and we show that they can be used to identify, characterize and quantify proteins and protein complexes with potential implications for structural biology, proteomics, biomarker detection and routine protein analysis.

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